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在血栓形成过程中,血小板衍生的微粒与纤维蛋白结合。

Platelet-derived microparticles associate with fibrin during thrombosis.

作者信息

Siljander P, Carpen O, Lassila R

机构信息

Wihuri Research Institute, Helsinki, Finland.

出版信息

Blood. 1996 Jun 1;87(11):4651-63.

PMID:8639834
Abstract

Platelet-derived microparticles (MP) are reported to express both pro- and anticoagulant activities. Nevertheless, their functional significance has remained unresolved. The present study monitored the generation and fate of MP in an experimental model of thrombosis with costimulation of platelets by collagen and thrombin. When minimally anticoagulated (0.5 micromol/L PPACK) blood was perfused over immobilized fibrillar type I collagen in a flow chamber at a low shear rate (300 s(-1)), endogenous thrombin was generated, as evidenced by thrombin-antithrombin III complex. In contrast to full anticoagulation 150 micromol/L PPACK) and the absence of collagen, large platelet aggregates and fibrin ensued during perfusions over collagen in the presence of thrombin. In these thrombi, MP, defined as GPIIbIIIa- and P-selectin-positive vesicles (<1 micron), were found to align fibrin in immunofluorescence and scanning immunoelectron microscopy. Moreover, in sections of embolectomized thromboemboli from patients GPIIbIIIa- and P-selectin-positive material compatible with MP was detected in a fibrin strand-like pattern. In vitro binding studies showed that MP bound to fibrin and acted there as procoagulants. In summary, we show that MP generated during thrombus formation associate with local fibrin. This adhesive function fibrin could imply a sustained modulatory role for MP in evolving thrombi.

摘要

据报道,血小板衍生微粒(MP)具有促凝血和抗凝血活性。然而,它们的功能意义仍未得到解决。本研究在胶原蛋白和凝血酶共同刺激血小板的血栓形成实验模型中监测了MP的产生和命运。当在流动腔室中以低剪切速率(300 s(-1))将最低抗凝(0.5 μmol/L PPACK)的血液灌注到固定化的I型纤维状胶原蛋白上时,如凝血酶-抗凝血酶III复合物所示,内源性凝血酶产生。与完全抗凝(150 μmol/L PPACK)和不存在胶原蛋白的情况相反,在凝血酶存在下灌注胶原蛋白期间会形成大量血小板聚集体和纤维蛋白。在这些血栓中,在免疫荧光和扫描免疫电子显微镜下发现,定义为GPIIbIIIa和P-选择素阳性的囊泡(<1微米)的MP可使纤维蛋白排列。此外,在来自患者的血栓切除术血栓栓塞切片中,在纤维蛋白条索样模式中检测到与MP相容的GPIIbIIIa和P-选择素阳性物质。体外结合研究表明,MP与纤维蛋白结合并在那里作为促凝剂起作用。总之,我们表明血栓形成过程中产生的MP与局部纤维蛋白相关。这种纤维蛋白的粘附功能可能意味着MP在不断发展的血栓中具有持续的调节作用。

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